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CN1051907A - 24-is with-VITAMIN-D-derivative, its preparation method; Contain the pharmaceutical preparation of this derivative and as the application of medicine - Google Patents

24-is with-VITAMIN-D-derivative, its preparation method; Contain the pharmaceutical preparation of this derivative and as the application of medicine Download PDF

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CN1051907A
CN1051907A CN90108993A CN90108993A CN1051907A CN 1051907 A CN1051907 A CN 1051907A CN 90108993 A CN90108993 A CN 90108993A CN 90108993 A CN90108993 A CN 90108993A CN 1051907 A CN1051907 A CN 1051907A
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derivative
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vitamin
hydrogen atom
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CN1031705C (en
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盖尔拉德·克舒
根特·尼夫
卡迪加·舒尔茨
马休斯·布劳迪格姆
露斯·瑟罗夫-埃克德
皮特·拉赫
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Bayer Pharma AG
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    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C401/00Irradiation products of cholesterol or its derivatives; Vitamin D derivatives, 9,10-seco cyclopenta[a]phenanthrene or analogues obtained by chemical preparation without irradiation
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    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
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Abstract

The new 24-that this paper has described formula I is with-VITAMIN-D-derivative,
And its a kind of preparation method, contain the pharmaceutical preparation of this compound and it is used to prepare the application of medicine.
This new compound has the effect that suppresses propagation and divide idioblast.

Description

24-is with-VITAMIN-D-derivative, its preparation method; Contain the pharmaceutical preparation of this derivative and as the application of medicine
The 24-that the present invention relates to the formula I is with-VITAMIN-D-derivative,
In the formula:
R 1Be a hydrogen atom, a hydroxyl or the acyloxy that 1 to 8 carbon atom is arranged,
R 2And R 3Be an alkyl that the straight chain of 1 to 4 carbon atom is arranged or side chain is arranged, a trifluoromethyl independently of one another or be a saturated carbon ring that 3 to 9 carbon atoms are arranged that links to each other with carbon atom 25 jointly,
R 4And R 5Be a hydrogen atom or the acyl group that 1 to 8 carbon atom is arranged independently of one another,
A and B respectively be a hydrogen atom or be one second key jointly,
N is 1,2,3,4 or 5,
The invention still further relates to said derivative the preparation method, contain these compounds pharmaceutical preparation with and for the application of making medicine.
May be as substituent R 1, R 4And R 5Acyloxy and acyl group particularly by saturated carboxylic acid or also by the benzoic acid deutero-.
If R 2And R 3With carbon atom 25 be a saturated carbocyclic ring jointly, then give special priority for the ring third the ring, the ring penta the ring or the hexamethylene ring.
The 24-of the preferred formula I of the present invention with-VITAMIN-D-derivative is,
R 1Be a hydroxyl,
R 2And R 3Be a methyl,
R 4And R 5Be a hydrogen atom and
N is 1,2 or 3.
A two key is preferably arranged between carbon atom 22 and 23.
Particularly preferred compound is
(5Z, 7E, 22E)-(24R)-9,10-seco-24a-is with-5,7 for 1S, 3R, 10(19), 22-courage steroid tetraene-1,3, the 24-triol and
(5Z, 7E, 22E)-(24S)-9,10-seco-24a-is with-5,7 for 1S, 3R, 10(19), and 22-courage steroid tetraene-1,3,24-triol.
Natural complex D 2And D 3And bioactive metabolites (natural complex D 2And D 3Itself be non-biological activity, after hydroxylation on 25 of liver or kidney 1, be only active) at C 10And C 19The position between the constitutional features of two keys as difference arranged, this pair key is to vitamins D activity play a decisive role (seeing the general formula V).Vitamins D 2And D 3Effect be to make plasma body Ca ++With plasma body phosphoric acid salt tamper stabilization, they suppress plasma body Ca ++The deposition of tamper.
Ergocalciferol: R a=R b=H, R c=CH 3, vitamins D 2
Two key C-22/23
Cholecalciferol: R a=R b=R c=H vitamins D 3
25-hydroxycholecalciferol: R a=R c=H, R b=OH
1a-hydroxycholecalciferol: R a=OH, R b=R c=H
1a, 25-dihydroxyl cholecalciferol: R a=R b=OH, R c=H
Calcitriol
Except obvious effect to calcium and phosphoric acid salt exchange of substance, vitamins D 2And D 3And the synthetic derivative also has effect (H, F, Deluca, vitamins D metabolism and the function in the steroid hormone biological chemistry, Hrsg, the H.L.Makin that suppresses propagation and distinguish cell, second edition, Blackwell Science Press, 1984, the 71-116 page or leaf).But when using vitamins D overtreatment phenomenon (hypercalcemia) may appear.
DE-AS2526981 disclosed at 24 hydroxylated 1a-cholecalciferols; Its toxicity is lower than not hydroxylated corresponding 1 α-cholecalciferol.Hydroxylated compound exhibits the selectivity activation of intestines calcium absorption and the bone resorption more weak than 1 α-cholecalciferol.
24-hydroxy vitamin-D-analogue of describing in the International Patent Application WO 87/00834 can be used for the treatment of humans and animals because abnormal cell proliferation and/or the caused obstacle of cytodifferentiation.
For various 1, the 25-dihydroxyl-with-VITAMIN-D-derivative, Deluca once mentioned the disassociation relevant with HL-60 cell differentiation character with bone resorption not long ago.Wherein, external bone resorption is directly measuring of the interior calcium mobilization of body.
Have now found that, compare that the 24-of formula I of the present invention has good surprising effect collection of illustrative plates with-VITAMIN-D-derivative with VITAMIN-D-derivative calcitriol (1a, 25-dihydroxyl cholecalciferol).When the influence for calcium and phosphoric acid salt exchange of substance obviously weakens (by overtreatment or require the high dosage effect of reduce paying), the effect that suppresses propagation and distinguish cell remain unchanged substantially (disassociation).
The VITAMIN of The compounds of this invention-D-activity is determined by means of the test of calcitriol acceptor.Carry out this test with a kind of by the special receptor protein that obtains in the rickety chicken intestines.In a test tube, be 0.575ml's with reaction volume 3The binding proteins matter that H-calcitriol (0.5ng/ml) will contain acceptor was cultivated 1 hour, and dividing has and do not wait to try two kinds of situations of material.There is not and is stained with the calcitriol of acceptor with charcoal-dextran absorption extraction.For this reason, add 200 μ l charcoal-dextran suspensions, and cultivated 30 minutes at 22 ℃ to each test tube.Then, centrifugation 10 minutes under 4 ℃ and 1500 * g condition.Precipitate and separate residuum, balance were used the atom optical measurement after 1 hour in a β counter.With different concns wait try material and reference substance (unlabelled calcitriol) obtains some repulsions 3The competition curve of the reference substance of H-mark, it is interrelated, find out a competition factor (KF).It is defined as the merchant that required the waiting of 50% competition tries material concentration and reference substance concentration:
KF=(substrate concentration to be tried during 50% competition)/(the reference substance concentration during 50% competition)
Therefore, (5Z, 7E, 22E)-(1S, 3R, 24R)-9,10-seco-24a-is with-5,7,10(19), 22-courage steroid tetraene-1,3, the KF value of 24-triol (compd A) is 67, (5Z, 7E, 22E)-(1S, 3R, 24S)-9,10-seco-24a-is with-5,7,10(19), 22-courage steroid tetraene-1,3, the KF value of 24-triol (compd B) is 0.8.
In order to determine the anti-proliferative capacity of The compounds of this invention, replace compd A and B as material to be tried, carried out following test:
Use Yuspa, S and Harris, C.C, improve one's methods " with the change differentiation of retinoic acid ester extracorporeal treatment mouse epidermic cell ", Exp.Cell Res.86:95-105,1974 preparations and cultivate the keratinocyte of newborn mouse.
Kill the newborn NMRI mouse of two kinds of sexes by broken end, peel off skin, in a kind of antibiotic-antimycotic agent solution, clean, with this side down in Dispase II solution (1.2U/ml in the M19.9 of tissue culturing medium+25mmol/L HEPS+15% fetus calf serum (FCS)+50U/ml penicillin/streptomycin (P/S) (preparation medium, PM)) cultivates a night down in 4 ℃.Take out epidermis, prepare single-cell suspension liquid by trypsinize.After the centrifugation, the cell deposition thing is suspended again, becomes and determine the small circle cell number of living after the trypanosome blueness, in Primaria 24 orifice plates and in the tissue culturing medium (M199+15%FCS+50U/ml P/S) with 4 * 10 5Cell/cm 2Density sowing cell.37 ℃ cultivate 24 hours after, wash cell in order to the salts solution (PBS) of phosphate buffered, again at 32.5 ℃ and have and do not wait to try to continue to cultivate 24 hours in the serum-free tissue culturing medium (M199,50U/ml P/S+0.5% ethanol) of material.Then, add 0.4 μ Ci/50 μ l 3H-methylthymidine (40Ci/mmol).Extract medium out after 4 hours, add ice-cold 10% Tricholroacetic Acid (TCA) of 500 μ l and finish reaction.Wash cell with TCA and PBS, and pass through at a kind of proteinase K-solution (10mmol/l three-HCl, 10mmol/lEDTA, 10mmol/l NaCl, 0.2%Triton-X100, PH8.0,50 μ g/ml protein kinases K) cultivate in and make it dissolving, and by centrifugation purification lysate.In residuum, determine radioactivity, DNA is carried out determining DNA concentration than after the dyeing with fluorescence photometric method with connection miaow Phenylindole (DAPI) with flicker photometric method.
Therefore, calcitriol and compd A are pressed used dosage with about identical IC with B 50Stop 3The H-thymidine enters DNA:
Calcitriol 2.7 * 10 -9Mol/l
Compd A 6.0 * 10 -9Mol/l
Compd B 9.5 * 10 -9Mol/l
Owing to reduced the danger of hypercalcemia, material of the present invention is applicable to that be the disease of feature with ad hoc fashion manufacturing treatment with the hyperplasia, for example excessively proliferative disease of skin (psoriasis) and malignant tumour (leukemia, colorectal carcinoma, mammary cancer).The precondition that success is treated is the calcitriol acceptor in the proof target tissue.
This compound can be mixed with the solution with acceptable solvent on the pharmacology, perhaps at suitable drug solvent or the emulsion in the carrier, suspension or dispersion liquid, perhaps is made into the pill, tablet or the capsule that contain solid carrier in a known way.For topical application, these compounds preferably are mixed with butterfat, paste or a kind of quasi-drugs form that is applicable to topical application.In this class preparation each can also contain other pharmaceutically acceptable and nontoxic auxiliary agent, for example stablizer, antioxidant, tackiness agent, pigment, emulsifying agent or seasonings.The sterile solution that the method for application of these compounds is preferably injected or intravenous injection is suitable, perhaps feed through oesophagus (digestive tube) as medicinal preparation for oral administration, or with butterfat, paste, washing lotion or suitable endermic plaster (endermic surgical adhesive sheet) form topical application, as described in EP-A-0387077.
The dosage of every day is
0.1 μ g(microgram)/patient/sky-1000 μ g(1mg)/patient/sky,
Preferably
1.0 μ patient g//sky-500 μ patient g//sky.
So compound of the present invention is also relevant with the pharmaceutical preparation of the compound that contains a kind of formula I at least and a kind of pharmacologically acceptable carrier.
In addition, the present invention relates to use the compound medicine of formula I.
According to the present invention, the 24-of formula I is preparation, that is: a kind of compound of general formula IV like this with-VITAMIN-D-derivative
Figure 901089931_IMG9
In the formula:
R 1' be a hydrogen atom or a protected hydroxyl,
R 4Be a hydroxy-protective group,
R 2And R 3And n is identical with formula I implication,
In case of necessity to 22, after the two keys of 23-carry out selective hydrogenation, change into a kind of compound of general formula III by 24-carbonyl functional group's reduction,
Figure 901089931_IMG10
R in the formula 1', R 4', R 2And R 3And the implication of n is identical with the formula IV,
A and B be one second key jointly or respectively be a hydrogen atom, and a kind of compound by making the general formula III with uviolizing is 5, and the two keys of 6-carry out vertical isomery conversion, are converted into a kind of compound of general formula II,
Figure 901089931_IMG11
R in the formula 1', R 4', R 2And R 3, n and A be identical with formula III implication with B, then, the hydroxy-protective group that exists by cracking and make where necessary oh group partly or entirely esterification change a kind of compound of formula I into.
General formula IV compound 24-carbonyl functional group's reduction for example uses Cerium II Chloride (III)/sodium borohydride to carry out in a kind of polar solvent.(24R) one of existing general formula III has (24S)-24-hydroxyl isomer to produce again during reduction.These two kinds of isomer can separate with chromatography.
Under the situation of needs, can be to C22 before carbonyl functional group's reduction, two keys of C23 carry out selective hydrogenation.
A kind of compound of general formula III then to the transformation of a kind of compound of general formula II for example by in the presence of alleged " triplet lens sensitizer ", carrying out with UV-irradiation.Within the scope of the invention, this has been used anthracene.By 5, the cracking of the two key π keys of 6-, A be around 5,6-singly-bound Rotate 180 ° and 5, and the reconstruction of the two keys of 6-has switched 5, the steric isomer of 6-pair of keys.
Then, the hydroxy-protective group that cracking exists preferably uses four-n-butyl Neutral ammonium fluoride and makes hydroxylic moiety or whole esterification freely by universal method with corresponding carboxylic acid halogenide (halogenide=muriate, bromide) or carboxylic acid anhydride when wishing.
By Calverley etc. at Tetrahedron 43,4609(1987) and the compound of type described in the International Patent Application WO 87/00834
Hydroxy-protective group R in the formula 1" and R 4" be dimethyl tertiary butyl silyl; The starting compound of preparation general formula IV; According to the present invention, also can imagine other trialkylsilkl and make the protection group.
Obtain the compound (witig reaction) of general formula IV with the positive phosphine reaction of formula VI.
Figure 901089931_IMG13
Following synthetic embodiment is used for further specifying the present invention.
The preparation of starting compound
I) isobutyl-carbonyl methylene tri phenyl phosphorane 1
A) brooethyl isobutyl ketone
The 50ml isobutyl methyl ketone is dissolved in the 240ml methyl alcohol, under 0 ℃, mix the 20ml bromine, and stirred 1.5 hours down at 10 ℃.Then add 360ml water, at room temperature stirred 16 hours.Use the saturated common salt solution diluted reaction mixture, separate organic phase, contain water with extracted with diethyl ether.Sodium carbonate solution washing with 10% merges the organic phase of getting up and uses the calcium chloride drying.After the filtration, evaporating solvent and distillation leftover.Obtain the 53.7g brooethyl isobutyl ketone of colorless oil; Kp 15-20Be 67-69 ℃.
B) isobutyl-carbonyl methyltriphenylphospbromide bromide phosphorus
53.6g brooethyl isobutyl ketone is added in the 78.5g triphenyl phosphine, made refrigerative reaction mixture recrystallization in methylene dichloride/ether (1: 2).Obtain the 111.7g fusing point and be 244-245 ℃ bromo-phosphonium.
C) isobutyl-carbonyl methylene tri phenyl phosphorane 1
111.6g isobutyl-carbonyl methyltriphenylphospbromide bromide phosphorus is dissolved in the 1500ml methylene dichloride, mix the NaOH of 1500ml 2N, at room temperature stirred 30 minutes.Isolate organic phase, the water flushing, and use dried over sodium sulfate.Behind filtration and the evaporating solvent, make resistates recrystallization in special fourth methyl ether.Obtain the 72.2g fusing point and be 120-121 ℃ title compound.By changing reactions steps ketone component a), can prepare other phosphorane of following formula in a similar manner.
II) (cyclopropyl methyl)-(triphenyl phosphoranediyl)-ketone 2
180mg lithium chloride and 540mg cupric chloride (I) were being stirred 1.5 hours under room temperature in the 9ml tetrahydrofuran (THF) in the presence of the nitrogen.After being cooled to 10 ℃, add the 15.0g(brooethyl that dissolves in the 225ml tetrahydrofuran (THF))-(triphenyl phosphoranediyl)-ketone (M.Le Corre, C.R.Acad.Sc.(C) 273,81(1971)), and stirred 30 minutes.Then, splash into the solution (G.F.Reynolds etc., organic chemistry magazine, 23,1217(1958)) of 1.6 volumetric molar concentrations that 29.5ml cyclopropyl bromination magnesium forms in tetrahydrofuran (THF), and under uniform temp, stirred 1.5 hours.In order to separate, reaction mixture is poured in ice/saturated ammonium chloride solution, then use ethyl acetate extraction.With sodium sulfate is the organic phase dehydration, concentrates then.With the silica gel chromatography separate solid residuum of band vinyl acetic monomer/acetone (3: 1), obtain the 5.6g fusing point and be 152 ℃ title compound 2.
III) (5E, 7E, 22E)-(1S, 3R)-1,3-is two-(tertiary butyl dimethyl-silicon alcoxyl base)-9, and 10-seco-24a-is with-5,7,10(19)-22-courage steroid tetraene-24-ketone 3
In the presence of 105 ℃ and nitrogen; with 8.0g(1S; 3R)-two-(tertiary butyl dimethyl-silicon alcoxyl base)-(20S)-formyl radical-9; pregnant steroid (the 5E of 10-seco; 7E; 10(19))-triolefin (Calverley Tetrahedron 43,4609(1987)) and 12.09 1 stirred 6 hours in the 46ml methyl-sulphoxide.Then, at room temperature use the vinyl acetic monomer diluted reaction mixture, and wash with salt solution.Make organic phase dehydration and filtration with sodium sulfate.After removing solvent, pass through the filtered through silica gel resistates with toluene.Boil off solvent and resistates is carried out gradient chromatographic separation (toluene/hexane (1 :) → toluene), produce 3.6g amorphous solid title compound 3 with silica gel.
(5E, 7E, 22E)-(1S, 3R)-1,3-pair-(tertiary butyl dimethyl-silicon alcoxyl base)-24-cyclopropyl methyl-9,10-seco bile-5,7,10(19), 22-tetraene-24-ketone 4
Reaction is carried out and is handled same II.
Reinforced: (20S)-formylation compound that 3.72g is identical with II,
5.6g 2; In the 21ml methyl-sulphoxide.
Product: 2.2g crystal buttery 4, fusing point: 97-98 ℃.
IV) (5E, 7E, 22E)-(24R)-1,3-is two for 1S, 3R-(tertiary butyl dimethyl-silicon alcoxyl base)-9, and 10-seco-24a-is with-5,7,10(19), 22-courage steroid tetraene-24-alcohol 5
V) (5E, 7E, 22E)-(24S)-1, two (the tertiary butyl dimethyl-silicon alcoxyl bases)-9 of 3-, 10-seco-24a-are with-5,7 for 1S, 3R, 10(19), and 22-courage steroid tetraene-24-alcohol 6
3.5g compound 3 is put into 9ml tetrahydrofuran (THF) and 20.6ml methyl alcohol, and with the methyl alcohol CeCl of a kind of 0.4 volumetric molar concentration of 20.6ml 37H 2O solution mixes.In nitrogen atmosphere and ice-cold condition, portioning adds the 570mg sodium borohydride.Suspension was stirred 40 minutes down ice-cooled again, be added in ice/salt solution then.Use the ethyl acetate extraction water, in the water and the washing organic phase, and dry on sodium sulfate.Filter and remove and desolvate, obtain 3.5g oil.Separate in the enterprising circumstances in which people get things ready for a trip spectrum of silica gel with vinyl acetic monomer/hexane (1: 9), obtain 534mg 5 and 692mg 6 as crystal oil.
(5E, 7E, 22E)-(1S, 3R, 24R)-1, and 3-pair-(tertiary butyl dimethyl-silicon alcoxyl base)-24-cyclopropyl methyl-9,10-seco bile-5,7,10(19), 22-tetraene-24-alcohol 7
(5E, 7E, 22E)-(1S, 3R, 24S)-1, and 3-pair-(tertiary butyl dimethyl-silicon alcoxyl base)-24-cyclopropyl methyl-9,10-seco bile 5,7,10(19), 22-tetraene-24-alcohol 8
The carrying out of reaction is identical with IV/V with processing.
Reinforced: the 2.2g in 5.8ml THF and 13.0ml methyl alcohol
4, the CeCl of 13.0ml 0.4 volumetric molar concentration 37H 2O
Solution, 359mg NaBH 4
2.22g oil is as crude product.
Product: 1.05g 7(and 8 lumps together),
330mg 8 is as resin.
Only describe 8 further conversion in the reaction below; 7 also can be similar to following manner continues processing.
VI) (5Z, 7E, 22E)-(24R)-1,3-is two for 1S, 3R-(tertiary butyl dimethyl-silicon alcoxyl base)-9, and 10-seco-24a-is with-5,7,10(19), 22-courage steroid tetraene-24-alcohol 9
Make 534mg 5 be dissolved in 75ml toluene, add 89mg anthracene and 1 triethylamine after, at room temperature use a high pressure mercury vapour lamp (Heraeus TQ150) to pass and send Simon Rex glass irradiation 5 minutes.Filter, concentrate muddy reaction mixture, and with vinyl acetic monomer/hexane (1: 9) chromatographic separation resistates on silica gel.Obtain 410mg buttery title compound.
VII) (5Z, 7E, 22E)-(24S)-1,3-is two for 1S, 3R-(tertiary butyl dimethyl-silicon alcoxyl base)-9, and 10-seco-24a-is with-5,7,10(19), 22-courage steroid tetraene-24-alcohol 10
The condition of simulation VI obtains 570mg buttery title compound by 680mg compound 6.
(5Z, 7E, 22E)-(1S, 3R, 24S)-1, and 3-pair-(tertiary butyl dimethyl-silicon alcoxyl base)-24-cyclopropyl methyl-9,10-seco bile-5,7,10(19), 22-tetraene-24-alcohol 11
320mg 8 is dissolved in the 45ml toluene, add 54mg anthracene and 1 triethylamine after, at room temperature use a high pressure mercury vapour lamp (Hereaus TQ150) to shine 5 minutes by send Simon Rex glass.Concentrated reaction mixture, resistates (375mg)-a kind of by 11 and the mixture formed of anthracene connect together with tetrabutyl ammonium fluoride and react.
Example 1
(5Z, 7E, 22E)-(24R)-9,10-seco-24a-is with-5,7 for 1S, 3R, 10(19), and 22-courage steroid tetraene-1,3,24-triol 12
Make 200mg compound 9 be dissolved in the 8.8ml tetrahydrofuran (THF), the solution of 1 volumetric molar concentration that itself and 1.5ml form by tetrabutyl ammonium fluoride and tetrahydrofuran (THF) was placed 50 minutes down at 60 ℃.Dilute cooled reaction mixture with vinyl acetic monomer, and wash with sodium hydrogen carbonate solution and salt solution.In the water and the washing organic phase, and dewater with sodium sulfate.Filter and evaporating solvent, form 210mg oil as resistates.With vinyl acetic monomer/hexane (2: 1) chromatographic separation on silica gel, obtain the title compound 12 of 124mg as amorphous solid.UV(MeOH)λ=210(ε=14720),264(14240)。
Example 2
(5Z, 7E, 22E)-(24S)-9,10-seco-24a-is with-5,7 for 1S, 3R, 10(19), and 22-courage steroid tetraene-1,3,24-triol 13
Under the condition of example 1, obtaining the 88mg fusing point by 200mg compound 10 is 128-129 ℃ title compound 13.
Example 3
(5Z, 7E, 22E)-(1S, 3R, 24S)-and 24-cyclopropyl methyl-9,10-seco bile-5,7,10(19), 22-tetraene-1,3,24-triol 14
Make the resistates of 375mg 11 be dissolved in the 14.2ml tetrahydrofuran (THF), the solution that makes 1 volumetric molar concentration that itself and 2.39ml form by tetrabutyl ammonium fluoride and tetrahydrofuran (THF) was placed 60 minutes under 60 ℃ and nitrogen atmosphere.In order to separate, cooled reaction mixture is poured in the cold sodium hydrogen carbonate solution, then use ethyl acetate extraction.With sodium sulfate organic phase is dewatered, after filtering and boiling off solvent, obtain the resinoid resistates of 400mg.With vinyl acetic monomer/hexane (2: 1) chromatographic separation on silica gel, produce the 150mg fusing point and be 137-139 ℃ 14.
Example 4
(5Z, 7E, 22E)-(1S, 3R, 24S)-and 24-cyclopentyl-methyl-9,10-seco bile-5,7,10(19), 22-tetraene-1,3,24-triol (16)
I) isopentyl carbonyl methylene tri phenyl phosphorane 15
Be similar to the method for preparing isobutyl-carbonyl methylene tri phenyl phosphorane, obtaining fusing point by the isopentyl methyl ketone is 64-67 ℃ solid title compound 15.
II)-V) be similar to II in the example 1)-V) described method; by 5.69g(1S; 3R)-two-(tertiary butyl dimethyl-silicon alcoxyl base)-(20S)-formyl radical-9; 10-seco pregnane-(5E; 7E; 10(19))-and triolefin A and 8.93g isopentyl carbonyl methylene tri phenyl phosphorane 15, obtain fusing point and be 119-120.5 ℃ solid title compound 16.
Example 5
(5Z, 7E, 22E)-(1S, 3R, 24S)-and 24-cyclopentyl-methyl-9,10-seco bile-5,7,10(19), 22-tetraene-1,3,24-triol 18
I) cyclopentyl-methyl carbonyl methylene radical triphen phosphorane 17
Be similar to the described method of preparation isobutyl-carbonyl methylene radical triphen phosphorane, obtaining fusing point by cyclopentyl acetone is 84-87 ℃ crystal oily title compound 17.
II)-V), be similar to II in the example 1)-V) described order; by 3.50g(1S; 3R)-two-(tertiary butyl dimethyl-silicon alcoxyl base)-(20S)-formyl radical-9; 10-seco pregnane-(5E; 7E, 10(19))-to obtain fusing point be 90-93 ℃ solid title compound 18 for triolefin A and 5.68g17.
Example 6
(5Z, 7E, 22E)-(1S, 3R, 24R)-and 24-(2-second butyl)-9,10-seco bile-5,7,10(19), 22-tetraene-1,3,24-triol 25
Example 7
(5Z, 7E, 22E)-(1S, 3R, 24S)-and 24-(2-second butyl)-9,10-seco bile-5,7,10(19), 22-tetraene-1,3,24-triol 26
I) 4-ethyl-pentanoyl methylene tri phenyl phosphorane 19
A) ethyl-2-butylene-1(2)-nitrile 19a
With the 170g(2 mole) Malonic mononitrile, 10g ammonium acetate, 10g acetic acid and 100ml benzene is placed in the flask of a 1L together.Add the 172g(2 mole to it) diethyl acetone, and under situation about refluxing with a condenser, boiled very carefully 18 hours.After the benzene evaporation, resistates is put into the HCl of 1000ml 2n, use extracted with diethyl ether, tell organic phase, with saturated NaCl solution washing, by Na 2SO 4Dehydration also concentrates.Under the 18mmHg column condition, resistates is distilled 2 times.Obtain 19 of 96.7g colorless oil.
Boiling point: 66-68 ℃, IR ν (CN) 2240-2212cm -1
B) ethyl-2-butane nitrile 19b
Making 96.7g(886mMol with ethanol) to be supplemented to volume be 150ml to 4-ethyl-2-butylene-1(2)-nitrile 19a.Add the pd/ carbon of 2g10% to it, and 50 ℃ of hydrogenations 7 hours.With diatomite filtration reaction mixture and concentrated, with the HCl absorption of 400ml 2n, use extracted with diethyl ether, dehydration concentrates, and distills under vacuum.Obtain the material 19b of 50.5g colorless oil.
KP 6-845℃,NMR(300MHz)〔δ〕0.92(6H,t)1.5(5H,m)2.34(2H,d)
C) 4-ethyl-methyl-n-butyl ketone 19C
With 14.4g(600mMol) Mg considers to be worth doing and the 150ml diethyl ether is placed in the three-necked bottle together.Splash into 85.2g(600mMol to it) be dissolved in the methyl iodide in the 50ml ether.Then add 100ml benzene, and distill out a part of diethyl ether.Add 33.3g(300mMol) ethyl-2-butyl nitrile 19b, and reflux and boiled 5 hours.Use NH 4This reaction mixture of Cl solution hydrolysis is used extracted with diethyl ether; Wash with water, use Na 2SO 4Dehydration, concentrate and through a Vigreux column vacuum distilling.Obtain the 19C of 12.4g colorless oil.
KP 1654℃,IRν(CO)1730cm -1
NMR〔δ〕0.86(6H,t)1.30(4H,m)1.80(1H,m)2.13(3H,s)2.33(2H,d)
D) brooethyl-4-ethyl pentyl group ketone 19d
With 12g(93mMol) 4-ethyl-methyl-n-butyl ketone of being dissolved in 60ml methyl alcohol 0 ℃ down and 14.8g(93mMol) bromine mixes mutually, 0 ℃ of restir 30 minutes.Then under cooling conditions, add 100ml water, and at room temperature stirred 16 hours.With saturated salt solution diluted reaction mixture, use extracted with diethyl ether, use saturated NaHCO 3Washing is also used Na 2SO 4Drying and dehydrating.Boil off solvent and distillation leftover after the filtration.Obtain 13.4g brooethyl-4-ethyl pentyl group ketone 19d.
KP 1254℃
NMR(300MHz)〔δ〕0.86(6H,t)1.23(4H,m)1.86(1H,m)2.58(2H,d)3.88(2H,s)
E) 4-ethyl pentanoyl methyltriphenylphospbromide bromide phosphorus 19e
With 13.4g(65mMol) brooethyl-4-ethyl pentyl group ketone 19d is added to 17.3g(65mMol) in the triphenyl phosphine.Add the 76ml methylene dichloride after placement is spent the night again and reflux and boiled 30 minutes.80ml methylene dichloride/ether (3: 5) washing is used again with 110ml ether diluted reaction mixture in the cooling back.Obtain 26.4g bromo-phosphonium 19e.
NMR(300MHz)〔δ〕0.78(6H,t)1.20(4H,m)1.77(1H,m)2.87(2H,d)5.7(2H,d)7.78(15H,m)
F) 4-ethyl pentanoyl methylene tri phenyl phosphorane 19
With 26g(55mMol) be dissolved in the 4-ethyl pentanoyl methyltriphenylphospbromide bromide phosphorus 19e 5.04g(60mMol of 70ml methyl alcohol) be dissolved in the sodium bicarbonate dilution of 70ml water, at room temperature stirred 30 minutes.Reaction mixture is added in the entry, use dichloromethane extraction, separate organic phase, wash with water, use Na 2SO 4Dehydration also concentrates.Stir resistates with vinyl acetic monomer.Obtain 18.8g title compound 19.
NMR(300MHz) (δ) 0.93(6H, t) 1.52(4H, m) 2.31(1H, m) 2.48(2H, d) 3.94(1H, wide d) 7.48 and 7.88(15H, m)
II) (5E, 7E, 22E)-(1S, 3R)-1,3-pair-(tertiary butyl dimethyl-silicon alcoxyl base)-24-(2-ethyl-butyl)-9,10-seco bile-5,7,10(19), 22-tetraene-24-ketone (20)
With 3.4g(5.9mMol) (20S) carbamoyl compound A and 5.7g(14.7mMol) 19 in 100ml toluene, be heated to 80 ℃ of one nights of mistake.Then reaction mixture is added in the entry, tell organic phase,, use Na with the saturated common salt solution washing 2SO 4Dehydration also concentrates.On silica gel, use this oily resistates of toluene chromatographic separation.Obtain 1.1g oily compound 20.
NMR(300MHz)〔δ〕0.53(3H,S)0.79(24H)1.2(3H,d)4.17(1H,m)4.48(1H,m)4.81(2H,d)5.78(1H,d)5.98(1H,d)6.39(1H,d)6.62(1H,q)
III) (5E, 7E, 22E)-(1S, 3R, 24R)-1, and 3-pair-(tertiary butyl dimethyl-silicon alcoxyl base)-24-(2-ethyl-butyl)-9,10-seco bile-5,7,10(19), 22-tetraene-24-alcohol 21
(5E, 7E, 22E)-(1S, 3R, 24S)-1, and two (tertiary butyl dimethyl-silicon alcoxyl the base)-24-(2-ethyl-butyls of 3-)-9,10-seco bile-5,7,10(19), 22-tetraene-24-alcohol 22
The carrying out of reaction and processing are described with III example 1/2.
Reinforced: as 1.1g(1.6mMol) to be dissolved in 20 of 2.8ml THF and 6.3ml methyl alcohol
920mg(2.47mMol) be dissolved in the CeCl of 6.1ml methyl alcohol 3* 7H 2O
263mg(6.96mMol)NaBH 4
Product: buttery 340mg 21 and 140mg 22.
21 and 22NMR(300MHz)
〔δ〕0.50(3H,s)0.7-0.88(24H)4.05(1H,m)4.14(1H,m)4.48(1H,m)4.91(2H,d)5.32(1H,dd)5.47(1H,dd)5.77(1H,d)6.40(1H,d)
(IV) (5Z, 7E, 22E)-(1S, 3R, 24R)-1, and 3-pair-(tertiary butyl dimethyl-silicon alcoxyl base)-24-(2-ethyl-butyl)-9,10-seco bile-5,7,10(19), 22-tetraene-24-alcohol 23
340mg 21 is dissolved in 60ml toluene, adds 53mg(0.30mMol) behind anthracene and 1 triethylamine, at room temperature use a high pressure mercury vapour lamp (being selected from TQ150) to shine 5 minutes by send Simon Rex glass.Filter muddy reaction mixture, and concentrate.Obtain 340mg title compound 23.
(5Z, 7E, 22E)-(1S, 3R, 24S)-1, and two (tertiary butyl dimethyl-silicon alcoxyl the base)-24-(2-ethyl-butyls of 3-)-9,10-seco bile-5,7,10(19), 22-tetraene-24-alcohol 24
Be similar to IV) described condition, obtain 130mg buttery title compound 24 by 130mg compound 22.
V) compound 23 that 340mg is dissolved in the 10ml tetrahydrofuran (THF) descends to keep 1 hour at 55 ℃ at the 1n of tetrahydrofuran (THF) tetrabutyl ammonium fluoride with 2ml.Dilute cooled reaction mixture with vinyl acetic monomer, and wash with sodium hydrogen carbonate solution and salt solution.In the water and the washing organic phase, by sodium sulfate dehydration and concentrate., after chromatographic separation on the silica gel and evaporation concentration, also filter with vinyl acetic monomer with hexane absorption of residual excess.Obtain the title compound 25 of 110mg as amorphous solid.
Fusing point: 147-154 ℃.
(5Z, 7E, 22E)-(1S, 3R, 24S)-and the 24-(2-ethyl-butyl)-9,10-seco bile-5,7,10(19), 22-tetraene-1,3,24-triol 26
Under preparation 25 condition, obtaining the 40mg fusing point by 130mg compound 24 is 135-138 ℃ title compound 26.

Claims (10)

1, the 24-of formula I is with-VITAMIN-D-derivative
In the formula:
R 1Be a hydrogen atom, a hydroxyl or the acyloxy that 1 to 8 carbon atom is arranged,
R 2And R 3Be an alkyl that the straight chain of 1 to 4 carbon atom is arranged or side chain is arranged, a trifluoromethyl independently of one another or be a saturated carbon ring that 3 to 9 carbon atoms are arranged that links to each other with carbon atom 25 jointly,
R 4And R 5Be a hydrogen atom or the acyl group that 1 to 8 carbon atom is arranged independently of one another,
A and B respectively be a hydrogen atom or be one second key jointly,
N is 1,2,3,4 or 5.
2, according to the 24-of claim 1 with-VITAMIN-D-derivative, wherein R 1It is a hydroxyl.
3, according to the 24-of claim 1 with-VITAMIN-D-derivative, wherein R 4And R 5It respectively is a hydrogen atom.
4, according to the 24-of claim 1 with-VITAMIN-D-derivative, wherein R 2And R 3It respectively is a methyl.
5, according to the 24-of claim 1 with-VITAMIN-D-derivative, wherein A and B are common forms one second key.
6, according to the 24-of claim 1 with-VITAMIN-D-derivative, wherein n is 1.
7, (5Z, 7E, 22E)-(24R)-9,10-seco-24a-is with-5,7 for 1S, 3R, 10(19), 22-courage steroid tetraene-1,3, the 24-triol,
(5Z, 7E, 22E)-(24S)-9,10-seco-24a-is with-5,7 for 1S, 3R, 10(19), and 22-courage steroid tetraene-1,3,24-triol.
8, the 24-of preparation formula I is with the method for-VITAMIN-D-derivative,
R in the formula 1, R 2, R 3, R 4And R 5, A and B and n implication identical with claim 1, it is characterized in that, make a kind of compound of general formula IV
Figure 901089931_IMG4
In the formula:
R 1' be a hydrogen atom or a protected hydroxyl,
R 4' be a hydroxy-protective group,
R 2And R 3And n is identical with formula I implication,
In case of necessity to 22, after the two keys of 23-carry out selective hydrogenation, be converted into a kind of compound of general formula III by the reduction of 24-carboxyl functional group,
Figure 901089931_IMG5
R in the formula 1', R 4', R 2And R 3And n is identical with formula IV implication,
A and B are one second key or respectively are a hydrogen atom that a kind of compound of general formula III is by using UV-irradiation 5 jointly, and 6-switches steric isomer in two key places, thereby is transformed into a kind of compound of general formula II,
Figure 901089931_IMG6
R in the formula 1', R 4', R 2And R 3, n and A and B implication cotype III, then, hydroxy-protective group that cracking exists and part or all of esterified hydroxy groups where necessary make it change into a kind of compound of formula I.
9, pharmaceutical preparation is characterized in that, it contains compound and a kind of medicine acceptable carrier of at least a claim 1 to 7.
10, the compound of claim 1 to 7 is used to make medicine.
CN90108993A 1989-10-02 1990-10-01 24-homo-Vitamin-0-derivatives, process for preparing them, pharmaceutical preparation containing them and use as pharmaceuticals Expired - Fee Related CN1031705C (en)

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